Methods and devices for crossing chronic total occlusions Patent Grant Jacobs , et al. January 21, 2 [Jacobs; Peter Alan]

Methods and devices for crossing chronic total occlusions

Jacobs , et al. January 21, 2

Patent Grant 8632556

U.S. patent number 8,632,556 [Application Number 12/289,154] was granted by the patent office on 2014-01-21 for methods and devices for crossing chronic total occlusions. This patent grant is currently assigned to Bridgepoint Medical, Inc.. The grantee listed for this patent is Peter Alan Jacobs, Chad John Kugler, Matthew Jonathan Olson, Ross Arlen Olson, David B. Robinson. Invention is credited to Peter Alan Jacobs, Chad John Kugler, Matthew Jonathan Olson, Ross Arlen Olson, David B. Robinson.

United States Patent	8,632,556
Jacobs , et al.	January 21, 2014

Methods and devices for crossing chronic total occlusions

Abstract

The present disclosure is directed to a method of facilitating treatment via a vascular wall defining a vascular lumen containing an occlusion therein. The method may include providing an intravascular device having a distal portion and a longitudinal axis and inserting the intravascular device into the vascular lumen. The method may further include positioning the distal portion in the vascular wall, rotating the intravascular device about the longitudinal axis, and advancing the intravascular device within the vascular wall.

Inventors:

Jacobs; Peter Alan (Minneapolis, MN), Kugler; Chad John (Buffalo, MN), Olson; Matthew Jonathan (Crystal, MN), Olson; Ross Arlen (Anoka, MN), Robinson; David B. (Chanhassen, MN)

Applicant:

Name	City	State	Country	Type
Jacobs; Peter Alan Kugler; Chad John Olson; Matthew Jonathan Olson; Ross Arlen Robinson; David B.	Minneapolis Buffalo Crystal Anoka Chanhassen	MN MN MN MN MN	US US US US US

Assignee:

Bridgepoint Medical, Inc. (Plymouth, MN)

Family ID:

40579831

Appl. No.:

12/289,154

Filed:

October 21, 2008

Prior Publication Data


	Document Identifier	Publication Date
	US 20090124899 A1	May 14, 2009

Related U.S. Patent Documents


Application Number	Filing Date	Patent Number	Issue Date
60999879	Oct 22, 2007

Current U.S. Class:	606/159
Current CPC Class:	A61B 17/02 (20130101); A61B 17/22 (20130101); A61M 25/0068 (20130101); A61B 2017/22095 (20130101); A61B 2017/22094 (20130101); A61M 25/0069 (20130101); A61M 25/0045 (20130101); A61M 2025/0197 (20130101); A61B 2017/00469 (20130101); A61B 17/32002 (20130101)
Current International Class:	A61B 17/22 (20060101)
Field of Search:	;606/127,128,167,180,170,185,159 ;604/7,8,508,264,104,510,95.01

References Cited [Referenced By]

U.S. Patent Documents


4020829	May 1977	Willson et al.
4233983	November 1980	Rocco
4569347	February 1986	Frisbie
4581017	April 1986	Sahota
4621636	November 1986	Fogarty
4747821	May 1988	Kensey et al.
4762130	August 1988	Fogarty et al.
4774949	October 1988	Fogarty
4819634	April 1989	Shiber
4878495	November 1989	Grayzel
4976689	December 1990	Buchbinder et al.
4979939	December 1990	Shiber
4990134	February 1991	Auth
5071406	December 1991	Jang
5127917	July 1992	Niederhauser et al.
5161534	November 1992	Berthiaume et al.
5193546	March 1993	Shaknovich
5201753	April 1993	Lampropoulos et al.
5263493	November 1993	Avitall
5275610	January 1994	Eberbach
5324263	June 1994	Kraus et al.
5356418	October 1994	Shturman
5372587	December 1994	Hammerslag et al.
5383856	January 1995	Bersin
5385152	January 1995	Abele et al.
5409453	April 1995	Lundquist et al.
5415637	May 1995	Khosravi
5464395	November 1995	Faxon et al.
5501667	March 1996	Verduin, Jr.
5505702	April 1996	Arney
5534007	July 1996	St Germain et al.
5555883	September 1996	Avitall
5571122	November 1996	Kelly et al.
5571169	November 1996	Plaia et al.
5603720	February 1997	Kieturakis
5643298	July 1997	Nordgren et al.
5645529	July 1997	Fagan et al.
5655548	August 1997	Nelson et al.
5695506	December 1997	Pike et al.
5728133	March 1998	Kontos
5741270	April 1998	Hansen et al.
5741429	April 1998	Donadio, III et al.
5759172	June 1998	Weber et al.
5779721	July 1998	Nash
5807241	September 1998	Heimberger
5824071	October 1998	Nelson et al.
5830222	November 1998	Makower
5830224	November 1998	Cohn et al.
5843050	December 1998	Jones et al.
5882329	March 1999	Patterson et al.
5910133	June 1999	Gould et al.
5916194	June 1999	Jacobsen et al.
5935108	August 1999	Katoh et al.
5944686	August 1999	Patterson et al.
5954713	September 1999	Newman et al.
5957900	September 1999	Ouchi
5968064	October 1999	Selmon et al.
5989276	November 1999	Houser et al.
6010449	January 2000	Selmon et al.
6013055	January 2000	Bampos et al.
6015405	January 2000	Schwartz et al.
6022343	February 2000	Johnson et al.
6033414	March 2000	Tockman et al.
6036707	March 2000	Spaulding
6036717	March 2000	Mers Kelly et al.
6059750	May 2000	Fogarty et al.
6068638	May 2000	Makower
6071281	June 2000	Burnside et al.
6071292	June 2000	Makower et al.
6081738	June 2000	Hinohara et al.
6099542	August 2000	Cohn et al.
6120516	September 2000	Selmon et al.
6126649	October 2000	VanTassel et al.
6155264	December 2000	Ressemann et al.
6157852	December 2000	Selmon et al.
6159225	December 2000	Makower
6183432	February 2001	Milo
6186972	February 2001	Nelson et al.
6190353	February 2001	Makower et al.
6203559	March 2001	Davis et al.
6217527	April 2001	Selmon et al.
6217549	April 2001	Selmon et al.
6221049	April 2001	Selmon et al.
6231546	May 2001	Milo et al.
6231587	May 2001	Makower
6235000	May 2001	Milo et al.
6241667	June 2001	Vetter et al.
6246914	June 2001	de la Rama et al.
6254588	July 2001	Jones et al.
6258052	July 2001	Milo
6266550	July 2001	Selmon et al.
6277133	August 2001	Kanesaka
6283940	September 2001	Mulholland
6283951	September 2001	Flaherty et al.
6283983	September 2001	Makower et al.
6287317	September 2001	Makower et al.
6302875	October 2001	Makower et al.
6330884	December 2001	Kim
6337142	January 2002	Harder et al.
6358244	March 2002	Newman et al.
6375615	April 2002	Flaherty et al.
6379319	April 2002	Garibotto et al.
6387119	May 2002	Wolf et al.
6398798	June 2002	Selmon et al.
6416523	July 2002	Lafontaine
6428552	August 2002	Sparks
6432127	August 2002	Kim et al.
6447539	September 2002	Nelson et al.
6475226	November 2002	Belef et al.
6482216	November 2002	Hiblar et al.
6485458	November 2002	Takahashi
6491660	December 2002	Guo et al.
6491707	December 2002	Makower et al.
6506178	January 2003	Schubart et al.
6508824	January 2003	Flaherty et al.
6508825	January 2003	Selmon et al.
6511458	January 2003	Milo et al.
6514217	February 2003	Selmon et al.
6544230	April 2003	Flaherty et al.
6561998	May 2003	Roth et al.
6565583	May 2003	Deaton et al.
6569143	May 2003	Alchas et al.
6569145	May 2003	Shmulewitz et al.
6569150	May 2003	Teague et al.
6579311	June 2003	Makower
6589164	July 2003	Flaherty
6599304	July 2003	Selmon et al.
6602241	August 2003	Makower et al.
6613081	September 2003	Kim et al.
6616675	September 2003	Evard et al.
6623448	September 2003	Slater
6638247	October 2003	Selmon et al.
6638293	October 2003	Makower et al.
6655386	December 2003	Makower et al.
6656195	December 2003	Peters et al.
6660024	December 2003	Flaherty et al.
6669709	December 2003	Cohn et al.
6685648	February 2004	Flaherty et al.
6685716	February 2004	Flaherty et al.
6694983	February 2004	Wolf et al.
6709444	March 2004	Makower
6719725	April 2004	Milo et al.
6726677	April 2004	Flaherty et al.
6746426	June 2004	Flaherty et al.
6746462	June 2004	Selmon et al.
6746464	June 2004	Makower
6786884	September 2004	DeCant, Jr. et al.
6800085	October 2004	Selmon et al.
6824550	November 2004	Noriega et al.
6830577	December 2004	Nash et al.
6837868	January 2005	Fajnztajn
6860892	March 2005	Tanaka et al.
6863684	March 2005	Kim et al.
6866676	March 2005	Kieturakis et al.
6884225	April 2005	Kato et al.
6905505	June 2005	Nash et al.
6929009	August 2005	Makower et al.
6936056	August 2005	Nash et al.
6942641	September 2005	Seddon
6949125	September 2005	Robertson
6991617	January 2006	Hektner et al.
7004173	February 2006	Sparks et al.
7025758	April 2006	Klint
7056325	June 2006	Makower et al.
7059330	June 2006	Makower et al.
7083588	August 2006	Shmulewitz et al.
7094230	August 2006	Flaherty et al.
7105031	September 2006	Letort
7134438	November 2006	Makower et al.
7137990	November 2006	Hebert et al.
7159592	January 2007	Makower et al.
7179270	February 2007	Makower
7191015	March 2007	Lamson et al.
7229421	June 2007	Jen et al.
7316655	January 2008	Garibotto et al.
7377910	May 2008	Katoh et al.
7465286	December 2008	Patterson et al.
7485107	February 2009	DiFiore et al.
2001/0000041	March 2001	Selmon et al.
2001/0056273	December 2001	Ewers
2002/0029052	March 2002	Evans et al.
2002/0052637	May 2002	Houser et al.
2002/0103459	August 2002	Sparks et al.
2003/0028200	February 2003	Berg et al.
2003/0040737	February 2003	Merril et al.
2003/0109809	June 2003	Jen et al.
2003/0120195	June 2003	Milo et al.
2003/0167038	September 2003	Yozu et al.
2003/0236542	December 2003	Makower
2004/0015193	January 2004	Lamson et al.
2004/0059280	March 2004	Makower et al.
2004/0102719	May 2004	Keith et al.
2004/0133225	July 2004	Makower
2004/0158143	August 2004	Flaherty et al.
2004/0167554	August 2004	Simpson et al.
2004/0230156	November 2004	Schreck et al.
2004/0249277	December 2004	Kato et al.
2004/0249338	December 2004	DeCant, Jr. et al.
2005/0038467	February 2005	Hebert et al.
2005/0049574	March 2005	Petrick et al.
2005/0171478	August 2005	Selmon et al.
2005/0177105	August 2005	Shalev
2005/0216044	September 2005	Hong
2005/0261663	November 2005	Patterson et al.
2006/0094930	May 2006	Sparks et al.
2006/0135984	June 2006	Kramer et al.
2006/0229646	October 2006	Sparks
2006/0271078	November 2006	Modesitt
2007/0083220	April 2007	Shamay
2007/0088230	April 2007	Terashi et al.
2007/0093779	April 2007	Kugler et al.
2007/0093780	April 2007	Kugler et al.
2007/0093781	April 2007	Kugler et al.
2007/0093782	April 2007	Kugler et al.
2007/0093783	April 2007	Kugler et al.
2007/0265596	November 2007	Jen et al.
2008/0103443	May 2008	Kabrick et al.
2008/0228171	September 2008	Kugler et al.
2008/0243065	October 2008	Rottenberg et al.
2008/0243067	October 2008	Rottenberg et al.
2009/0088685	April 2009	Kugler et al.
2009/0209910	August 2009	Kugler et al.
2009/0270890	October 2009	Robinson et al.
2010/0063534	March 2010	Kugler et al.
2010/0069945	March 2010	Olson et al.

Foreign Patent Documents


WO 0178822	Oct 2001	WO
WO 2007/033052	Mar 2007	WO
WO 2007/082216	Jul 2007	WO
WO 2008/063621	May 2008	WO
WO 2008/116600	Oct 2008	WO
WO 2009/054943	Apr 2009	WO
WO 2009/100129	Aug 2009	WO
WO 2009/134346	Nov 2009	WO
WO 2010/019241	Feb 2010	WO
WO 2010/044816	Apr 2010	WO

Other References

International Preliminary Report On Patentability for PCT/US08/11976 issued on Jan. 13, 2009 (7 pages). cited by applicant .
International Search Report for PCT/US08/11976 issued on Jan. 13, 2009 (1 page). cited by applicant .
Colombo, Antonio et al., Treating Chronic Total Occlusions Using Subintimal Tracking and Reentry: The STAR Technique, Catheterization and Cardiovascular Interventions, vol. 64:407-411 (2005). cited by applicant .
English translation of claims granted in European Application No. 08734691.2 (European national phase of WO 2008/116600 A1), dated Feb. 3, 2012 (3 pages). cited by applicant .
Extended European Search Report for European Application No. 08841515.3, dated Mar. 30, 2012 (6 pages). cited by applicant.

Primary Examiner: Severson; Ryan
Assistant Examiner: Papeika; Rachel S
Attorney, Agent or Firm: Seager, Tufte & Wickhem, LLC

Parent Case Text

CROSS-REFERENCE TO RELATED APPLICATION

This application claims the benefit of U.S. Provisional Application No. 60/999,879, filed Oct. 22, 2007, which is herein incorporated by reference in its entirety.

Claims

What is claimed is:

1. A method of treating a blood vessel with an intravascular device, the blood vessel having a vascular wall defining a vascular lumen containing an occlusion therein, the occlusion being disposed between a proximal segment of the vascular lumen and a distal segment of the vascular lumen, the method comprising: inserting the intravascular device into the vascular lumen, the intravascular device including a shaft defining a longitudinal axis and a tip located at a distal end of the shaft, wherein an outer diameter of the tip is greater than a diameter of the distal end of the shaft, a proximal portion of the tip tapering towards the shaft, and wherein the intravascular device defines a device lumen; rotating the intravascular device about the longitudinal axis to produce relative motion at an interface between the tip and surrounding tissue; advancing the tip out of the proximal segment of the vascular lumen into the vascular wall; advancing the intravascular device within the vascular wall to establish a channel in the vascular wall extending longitudinally across the occlusion; advancing the tip of the intravascular device into the distal segment of the vascular lumen distal of the occlusion; positioning a guidewire through the device lumen and into the vascular lumen beyond the occlusion; and withdrawing the intravascular device over the guidewire.

2. The method of claim 1, wherein the intravascular device is rotated at least a plurality of revolutions at a rotational speed between about 2 revolutions per minute and about 200 revolutions per minute.

3. The method of claim 2, wherein the intravascular device is rotated at a rotational speed between about 50 revolutions per minute and about 150 revolutions per minute.

4. The method of claim 1, further including stopping rotating and advancing the intravascular device when the tip of the intravascular device is advanced beyond the occlusion in the vascular lumen.

5. The method of claim 1, wherein rotating and advancing the intravascular device occur simultaneously.

6. The method of claim 1, wherein rotating the intravascular device includes rotating the entire intravascular device.

7. The method of claim 1, wherein rotating the intravascular device includes manually rotating a handle assembly positioned about the intravascular device.

8. The method of claim 1, wherein rotating the intravascular device includes rotating the intravascular device with an electric motor.

9. The method of claim 1, further including penetrating an intima of the vascular wall at a first location proximal to the occlusion in the vascular lumen and dissecting a layer of the wall.

10. The method of claim 1, further including penetrating the intima of the vascular wall at a second location distal to the occlusion in the vascular lumen.

11. The method of claim 1, further comprising positioning the tip in the vascular wall between an adventitia of the vascular wall and an intima of the vascular wall.

12. The method of claim 1, further comprising positioning the tip in the vascular wall between an adventitia of the vascular wall and the occlusion in the vascular lumen.

13. The method of claim 1, wherein the channel extends between the proximal segment and the distal segment.

14. The method of claim 1, wherein the tip has a flat distal face.

15. A method of treating a blood vessel with an intravascular device, the blood vessel having a vascular wall defining a vascular lumen containing an occlusion therein, the occlusion being disposed between a proximal segment of the vascular lumen and a distal segment of the vascular lumen, the method comprising: inserting an intravascular device into the vascular lumen, the intravascular device having a radiopaque marker, the intravascular device including a shaft defining a longitudinal axis and a tip located at a distal end of the shaft, wherein an outer diameter of the tip is greater than a diameter of the distal end of the shaft, a proximal portion of the tip tapering towards the shaft, the tip having a flat distal face, and wherein the intravascular device defines a device lumen; advancing the tip between the occlusion and an adventitia of the vascular wall; rotating the intravascular device to produce relative motion at an interface between the tip and surrounding tissue; advancing the tip between the adventitia and an intima of the vascular wall to a location distal of the occlusion; advancing the tip into the distal segment of the vascular lumen from the location distal of the occlusion; positioning a guidewire through the device lumen and into the vascular lumen beyond the occlusion; and withdrawing the intravascular device over the guidewire.

16. The method of claim 15, wherein receiving visual feedback confirming the rotation of the intravascular device includes: determining a first appearance of the radiopaque marker; determining a second appearance of the radiopaque marker; and alternating the radiopaque marker between the first appearance and the second appearance.

17. The method of claim 16, wherein the first appearance of the radiopaque marker includes a face having a width and a length, and the second appearance of the radiopaque marker includes an edge having the length and a thickness.

18. The method of claim 17, wherein the thickness is smaller than the length and the width.

19. The method of claim 17, wherein an area of the face is greater than an area of the edge.

20. The method of claim 15, further including positioning the tip in the vascular wall.

21. The method of claim 20, wherein positioning the tip in the vascular wall includes positioning the tip between the adventitia of the vascular wall and the intima of the vascular wall.

22. The method of claim 20, wherein positioning the tip in the vascular wall includes positioning the tip between the adventitia of the vascular wall and the occlusion in the vascular lumen.

23. The method of claim 15, further including advancing the intravascular device to establish a channel in the vascular wall extending longitudinally across the occlusion.

24. The method of claim 23, wherein the channel extends between the proximal segment and the distal segment.

25. The method of claim 15, wherein the intravascular device is rotated at least a plurality of revolutions.

26. The method of claim 25, wherein the intravascular device is rotated at a rotational speed between about 50 revolutions per minute and about 150 revolutions per minute.

27. A method of treating a blood vessel with an intravascular device, the blood vessel having a vascular wall defining a vascular lumen containing an occlusion therein, the occlusion being disposed between a proximal segment of the vascular lumen and a distal segment of the vascular lumen, the method comprising: positioning the intravascular device proximate the occlusion, the intravascular device including a shaft defining a longitudinal axis and a tip located at a distal end of the shaft, wherein an outer diameter of the tip is greater than a diameter of the distal end of the shaft, a proximal portion of the tip transitioning toward the diameter of the shaft, the intravascular device including a handle assembly disposed about the shaft, the handle assembly having a first portion and a second portion, and wherein the intravascular device defines a device lumen; rotating the first portion of the handle assembly relative to the second portion thus causing the handle assembly to grip the shaft at a first location along the longitudinal axis and cause rotation of the tip; advancing the tip of the intravascular device within the vascular wall to a location within the vascular wall distal of the occlusion to establish a channel in the vascular wall extending longitudinally across the occlusion; advancing the tip into the distal segment of the vascular lumen from the location within the vascular wall distal of the occlusion; positioning a guidewire through the device lumen and into the vascular lumen beyond the occlusion; and withdrawing the intravascular device over the guidewire.

28. The method of claim 27, wherein the handle assembly further includes at least one grip sleeve.

29. The method of claim 28, wherein the at least one grip sleeve is a plurality of grip sleeves.

30. The method of claim 28, wherein the at least one grip sleeve is within the handle body.

31. The method of claim 27, wherein the handle assembly is located over a proximal portion of a shaft of the intravascular device.

32. The method of claim 27, wherein the channel extends between the proximal segment and the distal segment.

33. The method of claim 27, wherein the tip has a flat distal face.

34. The method of claim 33, wherein the flat distal face includes a central aperture.

35. The method of claim 27, wherein the tip is rotated at least a plurality of revolutions.

36. The method of claim 35, wherein the tip is rotated at a rotational speed between about 50 revolutions per minute and about 150 revolutions per minute.

37. A method of treating a blood vessel with an intravascular device, the blood vessel having a vascular wall defining a vascular lumen containing an occlusion therein, the occlusion being disposed between a proximal segment of the vascular lumen and a distal segment of the vascular lumen, the method comprising: inserting an intravascular device having a shaft with a longitudinal axis into the vascular lumen, wherein a tip is fixed to a distal end of the shaft, wherein an outer diameter of the tip is greater than a diameter of the distal end of the shaft, and a handle assembly is attached to a proximal end of the shaft, and wherein the intravascular device defines a device lumen; positioning the tip near the occlusion; advancing the tip between the occlusion and an adventitia of the vascular wall; rotating the handle assembly to cause rotation of the tip about the longitudinal axis between the occlusion and the adventitia while advancing the tip to a location distal of the occlusion; wherein rotating the handle assembly and advancing the tip occur simultaneously, the intravascular device being rotated at least a plurality of revolutions at a rotational speed between about 50 revolutions per minute and about 150 revolutions per minute; passing the tip into the distal segment of the vascular lumen from the location distal of the occlusion; positioning a guidewire through the device lumen and into the vascular lumen beyond the occlusion; and withdrawing the intravascular device over the guidewire.

38. The method of claim 37, further including stopping rotating and advancing the tip when the tip of the intravascular device is advanced beyond the occlusion in the vascular lumen.

39. The method of claim 37, further including penetrating an intima of the vascular wall at a first location proximal to the occlusion in the vascular lumen and dissecting a layer of the wall.

40. The method of claim 37, wherein the shaft includes a coil having a plurality of filars wound in a helical shape, the coil extending from the distal end of the shaft to the proximal end of the shaft, the intravascular device further including a hub fixed to the proximal end of the shaft and a sleeve extending from a distal end of the shaft and covering a portion of the coil.

41. The method of claim 40, wherein the intravascular device further includes a sheath having a proximal end and a distal end, and covering a portion of the coil and a portion of the sleeve, the proximal end of the sheath located proximal to the proximal end of the sleeve, and the distal end of the sheath located proximal to the distal end of the sleeve.

42. The method of claim 40, wherein the intravascular device further includes a tube body having a proximal end and a distal end, and covering a portion of the coil and a portion of the sleeve, the distal end of the tube body extending beyond the proximal end of the sleeve, and the proximal end of the tube body is fixed to the hub.

43. The method of claim 37, wherein the handle assembly is slidably positioned about the intravascular device.

44. The method of claim 37, where the handle assembly is located about the intravascular device, the handle assembly comprising: a handle body threadedly connected to a handle cap, the handle cap being configured to rotate relative to the handle body; and at least one member configured to grip a shaft of the intravascular device in response to a rotation of the handle cap relative to the handle body.

45. The method of claim 37, wherein a channel extends between the proximal segment and the distal segment.

46. The method of claim 37, wherein the tip has a proximal portion that tapers towards the shaft.

47. The method of claim 37, wherein the tip has a flat distal face.

Description

FIELD OF THE INVENTION

The inventions described herein relate to devices and associated methods for the treatment of chronic total occlusions. More particularly, the inventions described herein relate to devices and methods for crossing chronic total occlusions and establishing a pathway blood flow past the chronic total occlusions.

BACKGROUND OF THE INVENTION

Due to age, high cholesterol and other contributing factors, a large percentage of the population has arterial atherosclerosis that totally occludes portions of the patient's vasculature and presents significant risks to patient health. For example, in the case of a total occlusion of a coronary artery, the result may be painful angina, loss of cardiac tissue or patient death. In another example, complete occlusion of the femoral and/or popliteal arteries in the leg may result in limb threatening ischemia and limb amputation.

Commonly known endovascular devices and techniques are either inefficient (time consuming procedure), have a high risk of perforating a vessel (poor safety) or fail to cross the occlusion (poor efficacy). Physicians currently have difficulty visualizing the native vessel lumen, can not accurately direct endovascular devices toward the visualized lumen, or fail to advance devices through the lesion. Bypass surgery is often the preferred treatment for patients with chronic total occlusions, but less invasive techniques would be preferred.

Described herein are devices and methods employed to exploit the vascular wall of a vascular lumen for the purpose of bypassing a total occlusion of an artery. Exploitation of a vascular wall may involve the passage of an endovascular device into and out of said wall which is commonly and interchangeable described as false lumen access, intramural access, submedial access or in the case of this disclosure, subintimal access.

BRIEF SUMMARY

Described herein are devices and methods employed to exploit the vascular wall of a vascular lumen for the purpose of bypassing a total occlusion of an artery. Exploitation of a vascular wall may involve the passage of an endovascular device into and out of said wall which is commonly and interchangeable described as false lumen access, intramural access, submedial access or in the case of this disclosure, subintimal access.

In one aspect, the present disclosure is directed to a method of facilitating treatment via a vascular wall defining a vascular lumen containing an occlusion therein. The method may include providing an intravascular device having a distal portion and a longitudinal axis and inserting the intravascular device into the vascular lumen. The method may further include positioning the distal portion in the vascular wall, rotating the intravascular device about the longitudinal axis, and advancing the intravascular device within the vascular wall.

In another aspect, the present disclosure is direct to a device for facilitating treatment via a vascular wall defining a vascular lumen containing an occlusion therein. The device may include a shaft having a distal end and a proximal end. The shaft may include a coil having a plurality of filars wound in a helical shape, the coil extending from the distal end of the shaft to the proximal end of the shaft, and a sleeve, having a proximal end and a distal end, the sleeve extending from the distal end of the shaft and covering a portion of the coil. The device may further include a tip fixed to the distal end of the shaft, and a hub fixed to the proximal end of the shaft.

BRIEF DESCRIPTION OF THE FIGURES

FIG. 1 is a cross-sectional view of an artery.

FIG. 2 is an additional view of the artery shown in the previous figure.

FIG. 3 is an additional view of the artery shown in the previous figure.

FIG. 4 is an additional view of the artery shown in the previous figure.

FIG. 5 is a cross-sectional view of an artery.

FIG. 6 is an additional view of the artery shown in the previous figure.

FIG. 7 is a partial cross-sectional view of an exemplary crossing device.

FIG. 8 is a plan view showing an assembly including the crossing device shown in the previous figure.

FIG. 9 is a plan view of the assembly shown in the previous figure.

FIG. 10 is a cross-sectional view of the assembly shown in the previous figure.

FIG. 11 is a cross sectional view of the handle assembly shown in the previous figure.

FIG. 12 is a partial cross-sectional view showing a guidewire that is disposed in a lumen defined by a shaft of a crossing device.

FIG. 13 is an additional view of the guidewire and crossing device shown in the previous figure.

FIG. 14 is a plan view showing a heart including a coronary artery.

FIG. 15A is an enlarged view showing a portion of the heart shown in the previous figure.

FIG. 15B is an enlarged plan view of a crossing device shown in FIG. 15A.

FIG. 16A is an additional view showing a crossing device disposed in a heart.

FIG. 16B is an enlarged plan view of a crossing device shown in FIG. 16A.

FIG. 17A is an enlarged view showing a portion of a heart and a crossing device that is extending into a proximal segment of a coronary artery of the heart.

FIG. 17B is a representation of a fluoroscopic display produced when radiopaque fluid has been injected into the body from the distal end of a crossing device while the distal end of the crossing device is disposed in the true lumen of a coronary artery.

FIG. 18A is an enlarged view showing a portion of a heart and a crossing device that is extending into a proximal segment of a coronary artery of the heart.

FIG. 18B is a representation of a fluoroscopic display produced when radiopaque fluid has been injected into the body from the distal end of a crossing device while the distal end of the crossing device is disposed in the subintimal space of a coronary artery.

DETAILED DESCRIPTION OF EXEMPLARY EMBODIMENTS

The following detailed description should be read with reference to the drawings in which similar elements in different drawings are numbered the same. The drawings, which are not necessarily to scale, depict illustrative embodiments and are not intended to limit the scope of the invention.

FIG. 1 is a cross-sectional view of an artery 102 having a wall 126. In FIG. 1, wall 126 of artery 102 is shown having three layers. The outermost layer of wall 126 is the adventitia 105 and the innermost layer of wall 126 is the intima 107. The tissues extending between intima 107 and adventitia 105 may be collectively referred to as the media 109. For purposes of illustration, intima 107, media 109 and adventitia 105 are each shown as a single homogenous layer in FIG. 1. In the human body, however, the intima and the media each comprise a number of sub-layers. The transition between the external most portion of the intima and the internal most portion of the media is sometimes referred to as the subintimal space.

Intima 107 defines a true lumen 106 of artery 102. In FIG. 1, an occlusion 108 is shown blocking true lumen 106. Occlusion 108 divides true lumen 106 into a proximal segment 103 and a distal segment 104. A crossing device 120 is disposed in proximal segment 103 of true lumen 106. Crossing device 120 may be used to establish a channel between proximal segment 103 and distal segment 104. Crossing device 120 of FIG. 1 comprises a tip 124 that is fixed to a distal end of a shaft 122.

FIG. 2 is an additional view of artery 102 shown in the previous figure. In the embodiment of FIG. 2, the distal end of crossing device 120 has been advanced in a distal direction so that tip 124 is disposed in subintimal space 128. With reference to FIG. 2, it will be appreciated that tip 124 has passed through intima 107 and is disposed between intima 107 and adventitia 105 of artery 102. The embodiment of FIG. 2 and other embodiments described herewithin show access to the subintimal space 128 by way of example, not limitation, as the crossing device 120 may alternatively pass through the occlusion 108 thus remaining disposed in the true lumen 106.

In the embodiment of FIG. 2, shaft 122 of crossing device 120 defines a lumen 130. Lumen 130 may be used to deliver fluids into the body. For example, radiopaque fluid may be injected through lumen 130 and into subintimal space 128. In some useful embodiments, lumen 130 is dimensioned to receive a guidewire.

FIG. 3 is an additional view of artery 102 shown in the previous figure. In the embodiment of FIG. 3, the distal end of crossing device 120 has been advanced so that tip 124 has moved in an axial direction through subintimal space 128. With reference to FIG. 3, it will be appreciated that tip 124 has moved distally past occlusion 108. In FIG. 3, tip 124 is shown residing between intima 107 and adventitia 105 of artery 102. Axial advancement of tip 124 may cause blunt dissection of the layers forming wall 126 of artery 102. Alternatively, the tip may cause blunt dissection of the materials comprising the occlusion 108 (not shown).

In some useful methods in accordance with the present disclosure, crossing device 120 is rotated about it's longitudinal axis and moved in a direction parallel to it's longitudinal axis simultaneously. When this is the case, rotation of crossing device 120 may reduce resistance to the axial advancement of crossing device 120. These methods take advantage of the fact that the kinetic coefficient of friction is usually less than the static coefficient of friction for a given frictional interface. Rotating crossing device 120 assures that the coefficient of friction at the interface between the crossing device and the surround tissue will be a kinetic coefficient of friction and not a static coefficient of friction.

FIG. 4 is an additional view of artery 102 shown in the previous figure. In the embodiment of FIG. 4, crossing device 120 has been withdrawn from true lumen 106 of artery 102. With reference to FIG. 4, it will be appreciated that a guidewire 132 remains in the position formerly occupied by crossing device 120.

The position of guidewire 132 shown in FIG. 4 may be achieved using crossing device 120. Guidewire 132 may be positioned, for example, by first placing crossing device 120 in the position shown in the previous figure, then advancing guidewire 132 through lumen 130 defined by shaft 122 of crossing device 120. Alternately, guidewire 132 may be disposed within lumen 130 while crossing device 120 is advanced through the vasculature of a patient. When this is the case, guidewire 132 may be used to aid in the process of steering crossing device 120 through the vasculature.

With guidewire 132 in the position shown in FIG. 4, guidewire 132 may be used to direct other devices to subintimal space 128. For example, a catheter may be advanced over guidewire 132 until the distal end of the catheter is disposed in subintimal space 128. After reaching the subintimal space, the catheter may be used to dilate subintimal space 128. Examples of catheters that may be used to dilate the subintimal space include balloon catheters and atherectomy catheters.

FIG. 5 is a cross sectional view of an artery 202 having a wall 226. In FIG. 5, a crossing device 220 is shown extending through subintimal space 228 and around an occlusion 208. In FIG. 5, occlusion 208 is shown blocking a true lumen 206 defined by an intima 207 of wall 226. Occlusion 208 divides true lumen 206 into a proximal segment 203 and a distal segment 204. When a crossing member in accordance with some embodiments of the present disclosure is advanced through the subintimal space of an artery, the distal end of the crossing device may penetrate the intima and enter the distal segment of the true lumen after advancing beyond an occlusion.

In the embodiment of FIG. 5, a tip 224 of crossing device 220 is disposed in distal segment 204. Accordingly, it will be appreciated that crossing device 220 has pierced intima 207 distally of occlusion 208 and entered distal segment 204 of artery 202. In FIG. 5, shaft 222 is shown extending through intima 207 and subintimal space 228. Shaft 222 of crossing device 220 may define a lumen 230.

FIG. 6 is an additional view of artery 202 shown in the previous figure. In the embodiment of FIG. 6, crossing device 220 has been withdrawn leaving a guidewire 232 in the position shown in FIG. 6.

The position of guidewire 232 shown in FIG. 6 may be achieved using crossing device 220. Guidewire 232 may be positioned, for example, by first placing crossing device 220 in the position shown in the previous figure, then advancing guidewire 232 through lumen 230 defined by shaft 222 of crossing device 220. Alternately, guidewire 232 may be disposed within lumen 230 while crossing device 220 is advanced through the vasculature of a patient. When this is the case, guidewire 232 may be used to aid in the process of steering crossing device 220 through the vasculature of a patient.

Devices such as balloon angioplasty catheters and atherectomy catheters may be advanced over guidewire 232 and into subintimal space 228. In this way, these devices may be used in conjunction with guidewire 232 to establish a blood flow path between proximal segment 203 of true lumen 206 and distal segment 204 of true lumen 206. This path allows blood to flow through subintimal space 228 and around occlusion 208.

FIG. 7 is a partial cross-sectional view of an exemplary crossing device 320. Crossing device 320 of FIG. 7 comprises a tip 324 that is fixed to a distal end of a shaft 322. In the exemplary embodiment of FIG. 7, shaft 322 comprises a coil 334, a sleeve 336, a tubular body 338, and a sheath 344.

Tip 324 is fixed to a distal portion of coil 334. Coil 334 comprises a plurality of filars 342 that are wound in a generally helical shape. In some useful embodiments of crossing device 320, coil 334 comprises eight, nine or ten filars wound into the shape illustrated in FIG. 7. Crossing device 320 includes a sleeve 336 that is disposed about a portion of coil 334. Sleeve 336 may comprise, for example, PET shrink tubing, i.e. polyethylene terephthalate.

Sleeve 336 and coil 334 both extend into a lumen defined by a tubular body 338. Tubular body 338 may comprise, for example hypodermic tubing formed of Nitinol, i.e. nickel titanium. With reference to FIG. 7, it will be appreciated that a proximal portion of sleeve 336 is disposed between tubular body 338 and coil 334. In some embodiments of crossing device 320, a distal portion of tubular body 338 defines a helical cut. This helical cut may be formed, for example, using a laser cutting process. The helical cut may be shaped and dimensioned to provide an advantageous transition in lateral stiffness proximate the distal end of tubular body 338.

A proximal portion of coil 334 extends proximally beyond the distal end of tubular body 338. A hub 346 is fixed to a proximal portion of coil 334 and a proximal portion of tubular body 338. Hub 346 may comprise, for example, a luer fitting. Sheath 344 is disposed about a portion of tubular body 338 and a portion of sleeve 336. In some embodiments of crossing device 320, sheath 344 comprises HYTREL, a thermoplastic elastomer.

With reference to FIG. 7, it will be appreciated that tubular body 338, coil 334, sleeve 336, and sheath 344 each have a proximal end and a distal end. The proximal end of sheath 344 is disposed between the proximal end of tubular body 338 and the proximal end of sleeve 336. The distal end of sleeve 336 is positioned proximate tip 324 that is fixed to the distal end of coil 334. The distal end of sheath 344 is located between the distal end of tubular body 338 and the distal end of sleeve 336. With reference to FIG. 7, it will be appreciated that sheath 344 overlays the distal end of tubular body 338.

With reference to FIG. 7, it will be appreciate that tip 324 has a generally rounded shape. The generally rounded shape of tip 324 may reduce the likelihood that crossing device 320 will penetrate the adventitia of an artery. Tip 324 may be formed from a suitable metallic material including but not limited to stainless steel, silver solder, and braze. Tip 324 may also be formed from suitable polymeric materials or adhesives including but not limited to polycarbonate, polyethylene and epoxy. In some embodiments of crossing device 320, outer surface 340 of tip 324 comprises a generally non-abrasive surface. For example, outer surface 340 may have a surface roughness of 25 micrometers or less. A tip member having a relatively smooth outer surface may reduce the likelihood that the tip member will abrade the adventitia of an artery.

FIG. 8 is a plan view showing an assembly 348 including crossing device 320 shown in the previous figure. In the embodiment of FIG. 8, a handle assembly 350 is coupled to crossing device 320. In FIG. 8, handle assembly 350 is shown disposed about a proximal portion of shaft 322 of crossing device 320. Handle assembly 350 comprises a handle body 352 and a handle cap 354.

In some useful embodiments in accordance with the present disclosure, handle assembly 350 is long enough to receive the thumb and for fingers of a physician's right and left hands. When this is the case, a physician can use two hands to rotate handle assembly 350. In the embodiment of FIG. 8, grooves 356 are formed in handle body 352 and handle cap 354. Grooves 356 may improve the physician's ability to grip handle assembly 350.

FIG. 9 is an additional plan view showing assembly 348 shown in the previous figure. In FIG. 9, a proximal portion of handle assembly 350 is positioned between the thumb and forefinger of a left hand 358. A distal portion of handle assembly 350 is disposed between the thumb and forefinger of a right hand 360.

In some useful methods, crossing device 320 is rotated and axially advanced simultaneously. Rotation of crossing device 320 can be achieved by rolling handle assembly 350 between the thumb and forefinger one hand. Two hands can also be used as shown in FIG. 9. Rotating crossing device 320 assures that the coefficient of friction at the interface between the crossing device and the surround tissue will be a kinetic coefficient of friction and not a static coefficient of friction.

In some useful methods in accordance with the present disclosure, crossing device 320 is rotated at a rotational speed of 2 to 200 revolutions per minute. In some particularly useful methods in accordance with the present disclosure, crossing device 320 is rotated at a rotational speed of 50 and 150 revolutions per minute. Crossing device 320 may be rotated by hand as depicted in FIG. 9. It is also contemplated that a mechanical device (e.g., an electric motor) may be used to rotate crossing device 320.

FIG. 10 is a cross-sectional view of assembly 348 shown in the previous figure. With reference to FIG. 10 it will be appreciated that handle assembly 350 is disposed about sheath 344, tubular body 338, sleeve 336 and coil 334.

FIG. 11 is a cross sectional view of handle assembly 350 shown in the previous figure. With reference to FIG. 11, it will be appreciated that handle assembly 350 includes a plurality of grip sleeves 362 and a plurality of spacers 364. In the embodiment of FIG. 11, handle cap 354 includes male threads 366 that engage female threads 368 in handle body 352.

When handle cap 354 is rotated relative to handle body 352, the threads produce relative longitudinal motion between handle cap 354 and handle body 352. In other words, handle cap 354 can be screwed into handle body 352. As handle cap 354 is advanced into handle body 352, the inner end of handle cap 354 applies a compressive force to grip sleeves 362. Grip sleeves 362 are made from an elastomeric material. The compression forces applied to grip sleeves 362 by handle body 352 and handle cap 354 cause grip sleeves 362 to bulge. The bulging of grip sleeves 362 causes grip sleeves 362 to grip shaft 322 of crossing device 320.

The force that each grip sleeve 362 applies to the shaft is generally equally distributed about the circumference of the shaft. When this is the case, the likelihood that the shaft will be crushed by the grip sleeves is reduced. At the same time, the grip sleeves provide an interface that allows significant torque to be applied to the shaft when the handle is rotated.

FIG. 12 is a partial cross-sectional view showing a guidewire 432 that is disposed in a lumen 430 defined by a shaft 422 of a crossing device 420. FIG. 13 is an additional view showing guidewire 432 and crossing device 420 shown in FIG. 12. In some embodiments of crossing device 420, shaft 422 defines a lumen 430. When this is the case, a guidewire may be inserted into the lumen. The guidewire may be used to steer the crossing device. The guidewire may remain inside the lumen until it is needed for steering. When steering is needed, the guidewire may be advanced so that a portion of the guidewire extends beyond the distal end of the crossing device. A distal portion of the guidewire may then be advanced in the direction that the physician wishes to advance crossing device 420.

In the embodiment of FIG. 13, guidewire 432 has been distally advanced (relative to the position shown in FIG. 12). With reference to FIG. 13, it will be appreciated that a distal portion 470 of guidewire 432 is extending beyond the distal end of crossing device 420. In the embodiment of FIG. 13, distal portion 470 of guidewire 432 is biased to assume a generally curved shape when it is unrestrained by crossing device 420.

In the embodiment of FIG. 13, there are at least two degrees of freedom between guidewire 432 and crossing device 420. First, guidewire 432 and crossing device 420 are free to rotate relative to one another. Second, guidewire 432 and crossing device 420 are free to move in a longitudinal direction relative to one another. It is sometimes desirable to use guidewire 432 as an aid in directing crossing device 420 through the vasculature of a patient. When this is the case, distal portion 470 of guidewire 432 may be advanced beyond the distal end of crossing device 420. Guidewire 432 may then be rotated until distal portion 470 of guidewire 432 assumes a desired orientation.

FIG. 14 shows a heart 500 including a coronary artery 502. An occlusion 508 is disposed in coronary artery 502. Occlusion 508 divides a lumen of coronary artery 502 into a proximal segment 503 and a distal segment 504. The proximal segment 503 may be easily accessed using endovascular devices and has adequate blood flow to supply the cardiac muscle. The distal segment 504 is not easily accessed with interventional devices and has significantly reduced blood flow as compared to proximal segment 503.

FIG. 15A is an enlarged view showing a portion of heart 500 shown in the previous figure. In FIG. 15A, a crossing device 520 is disposed in proximal segment 503 of coronary artery 502. FIG. 15B is an enlarged plan view of crossing device 520 shown in FIG. 15A. Crossing device 520 comprises a tip 524 and a shaft 522.

FIG. 16A is an additional view showing crossing device 520 disposed in heart 500. FIG. 16B is an enlarged plan view of crossing device 520 shown in FIG. 16A. In FIGS. 16A and 16B crossing device 520 has been rotated approximately ninety degrees relative to the position shown in FIGS. 15A and 15B.

Some useful methods in accordance with the present disclosure include the step of rotating crossing device 520. When the proximal portion of a crossing device is rotated, it may be desirable to confirm that the distal end of the crossing device is also rotating.

Many physicians have experience using guidewires. These physicians are aware that twisting the proximal end of a guidewire when the distal end of the guidewire is fixed may cause the guidewire to break due to twisting. Accordingly, many physicians may be hesitant to rotate an intravascular device more than a few revolutions unless they are certain that the distal end of the device is free to rotate.

One method for determining whether the tip of a crossing member is rotating may be described with reference to FIGS. 15A, 15B, 16A and 16B. As shown in the figures, crossing member 520 comprises a tip 524 fixed to the distal end of a shaft 522. Tip 524 comprises a radiopaque marker 572. Radiopaque marker 572 has a face 574 and an edge 576. Face 574 has a width W and a length L. Edge 576 has a length L and a thickness T. In some useful embodiments of crossing device 520, thickness T of radiopaque marker 572 is smaller then both length L and width W. When this is the case, radiopaque marker 572 may be used to provide a physician with visual feedback indicating that tip 524 of crossing device 520 is rotating.

During rotation of crossing device 520, the shape of radiopaque marker provides visual feedback assuring the physician that the tip of the crossing member is rotating as the physician rotates the proximal portion of the crossing member. Radiopaque marker 572 provides two different appearances while it is being rotated and observed using fluoroscopic methods. When edge 576 of radiopaque marker is viewed on a fluoroscopic display a first appearance is achieved. When face 574 of radiopaque marker 572 is viewed, it provides a second appearance on the fluoroscopic display. With reference to the figures, it will be appreciate that the first appearance has a smaller footprint than the second appearance. When the appearance of radiopaque marker 572 is alternating between the first appearance and the second appearance, the physician can infer that tip 524 is rotating. This visual feedback allows the physician to confirm that the distal end of crossing member is rotating.

FIGS. 17A and 18A each show a crossing device 520 comprising a tip 524 fixed to a shaft 522. Tip 524 comprises a radiopaque marker 572. Tip 524 of crossing device 520 has been advanced through a proximal segment 503 of a coronary artery 502. With reference to FIGS. 17A and 18A, it will be appreciated that tip 524 is near wall 526 of coronary artery 502 and an occlusion 508 that is located in the true lumen of coronary artery 502. When a surgical procedure is viewed on a fluoroscope, it may be difficult for the physician to determine whether or not tip 524 is disposed in the subintimal space of coronary artery 502. Methods for determining whether the tip is disposed in the subintimal space may be described with reference to FIGS. 17 and 18.

For example, one method in accordance with the present disclosure may include the steps of positioning the distal end of a crossing device in a position that may or may not be in the subintimal space of an artery and injecting radiopaque fluid into the body from the distal end of crossing device 520. If the radiopaque fluid remains in a localized area (e.g., in the subintimal space) then a physician viewing the radiopaque fluid on a fluoroscopic display can infer that the distal end of the crossing device is disposed in the subintimal space. If the radiopaque fluid rapidly enters the bloodstream and is carried through the vasculature, then the physician can infer that the distal end of the crossing device is disposed in the true lumen of the artery.

FIG. 17B is a representation of a fluoroscopic display 578 produced when radiopaque fluid has been injected into the body from the distal end of crossing device 520 while tip 524 is disposed in the true lumen of coronary artery 502. In FIG. 17B, the radiopaque fluid 580 has rapidly entered the bloodstream and has cause the vasculature in fluid communication with proximal segment 503 to become illuminated on fluoroscopic display 578. Radiopaque marker 572 is also visible in fluoroscopic display 578.

FIG. 18B is a representation of a fluoroscopic display 578 produced when radiopaque fluid has been injected into the body from the distal end of crossing device 520 while tip 524 is disposed in the subintimal space of coronary artery 502. In FIG. 18B, the radiopaque fluid 580 is disposed in a localized area (i.e., in the subintimal space). Radiopaque marker 572 is also visible in fluoroscopic display 578.

Additional methods are also contemplated. For example, negative pressure (i.e., sub atmospheric pressure) may be applied to the lumen defined by crossing device 520. The physician may observe the results of this application of negative pressure. If a partial vacuum is produced and little or no blood is drawn through the lumen, then the physician can infer that the distal end of the lumen is located in the subintimal space. If, on the other hand, blood is drawn through the lumen of the crossing member, then the physician can infer that the distal end of the crossing member is disposed in the true lumen of a blood vessel.

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